Abstract

Human infants develop opiate dependence and undergo withdrawal if they are exposed in utero to illicit drugs such as heroin, or to prescribed opiates such as methadone, or ex utero when treated with opiates for pain. To devise rationale treatments for this abstinence syndrome, and to understand the long term consequences of opiate dependence in the neonate, it is necessary to understand more fully how these drugs act on the neurobehavioral systems of the neonate. Until recently the only detailed description of an opiate abstinence syndrome in neonates was for humans. The complexity of the human setting made it impossible to tease apart those factors that are due to opiate use and those that are due to the abuse of other drugs, poor prenatal care, undernutrition, or any of the other complications experienced by the mothers of these children. The first and necessary step in this process, to describe the phenomenology of precipitated withdrawal in infants, has been accomplished. Two groups, including ours, have detailed an opiate withdrawal syndrome, in the infant rat, that includes behaviors such as head swaying, stretching, rolling, and the inability to stay quiet. Aspects of this syndrome are seen even in the fetus, and the withdrawal syndrome slowly changes over development to reach, around puberty, the classic constellation of withdrawal behaviors so often described for the adult animal. Furthermore, the dysphoria associated with abstinence appears in the infant rat, but develops later, around 14 days of age, dissociating the unconditioned """"""""physical"""""""" withdrawal signs from the affective component of abstinence. Because the withdrawal syndrome in the infant is now described in great detail, we are poised to ask a number of questions that could not have been addressed even two years ago. The experiments in this proposal examine where and how this syndrome is organized in the brain, and what are the developmental continuities and discontinuities in the neural substrates of opiate withdrawal, describes changes in state regulation that may occur during normal development and under conditions of stress, and begins to study pharmacologic treatments, both clinically approved and experimental, of the opiate abstinence syndrome in the neonate. The data from these experiments shall provide a detailed knowledge of the neural and physiological underpinnings of the neonatal abstinence syndrome, in all its complexity, and represents the first efforts to investigate pharmacologic therapies that might be used to ameliorate the expression of opiate withdrawal in the infant.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Drug Abuse (NIDA)
Type
Research Project (R01)
Project #
5R01DA006600-10
Application #
6174630
Study Section
Human Development Research Subcommittee (NIDA)
Program Officer
Thadani, Pushpa
Project Start
1989-09-30
Project End
2002-01-31
Budget Start
2000-08-01
Budget End
2002-01-31
Support Year
10
Fiscal Year
2000
Total Cost
$129,740
Indirect Cost

  Institution

Name
New York State Psychiatric Institute
Department
Type
DUNS #
167204994
City
New York
State
NY
Country
United States
Zip Code
10032

  Publications

Barr, Gordon A; McPhie-Lalmansingh, Anika; Perez, Jessica et al. (2011) Changing mechanisms of opiate tolerance and withdrawal during early development: animal models of the human experience. ILAR J 52:329-41
McPhie, Anika A; Barr, Gordon A (2009) Regional Fos expression induced by morphine withdrawal in the 7-day-old rat. Dev Psychobiol 51:544-52
Butkevich, Irina P; Barr, Gordon A; Vershinina, Elena A (2007) Sex differences in formalin-induced pain in prenatally stressed infant rats. Eur J Pain 11:888-94
Butkevich, I P; Barr, G A; Vershinina, E A (2007) [Sex-dependent differences in parameters of a long-term pain caused by inflammatory focus in prenatally stressed newborn rats] Zh Evol Biokhim Fiziol 43:54-9
Butkevich, Irina P; Barr, Gordon A; Mikhailenko, Victor A et al. (2006) Increased formalin-induced pain and expression of fos neurons in the lumbar spinal cord of prenatally stressed infant rats. Neurosci Lett 403:222-6
Zhu, Hongbo; Barr, Gordon A (2003) Ontogeny of NMDA receptor-mediated morphine tolerance in the postnatal rat. Pain 104:437-47
Jones, Kathy L; Zhu, Hongbo; Jenab, Shirzad et al. (2002) Attenuation of acute morphine withdrawal in the neonatal rat by the competitive NMDA receptor antagonist LY235959. Neuropsychopharmacology 26:301-10
Jones, K L; Barr, G A (2001) Injections of an opioid antagonist into the locus coeruleus and periaqueductal gray but not the amygdala precipitates morphine withdrawal in the 7-day-old rat. Synapse 39:139-51
Zhu, H; Barr, G A (2001) Opiate withdrawal during development: are NMDA receptors indispensable? Trends Pharmacol Sci 22:404-8
Zhu, H; Barr, G A (2001) Inhibition of morphine withdrawal by the NMDA receptor antagonist MK-801 in rat is age-dependent. Synapse 40:282-93

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